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Immunity to infectious diseases.

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Title: Immunity to infectious diseases.

1
Immunity to infectious diseases.

Prof. Mohamed Osman Gad El Rab.
College of Medicine KKUH.

2
Classification of immunity.

Acquired immunity.
active.
passive.
natural. artificial. natural.
artificial.
infections. immuniz. Maternal immuno
-
IgG.
therapy.

Immunity to viral infections .

Innate (natural) immunity
many viruses induce
1. production of type 1 interferons.
( INF- alpha INF - beta.)
2. activation of NK - cells .

5
dsRNA produced during viralreplication
induce the expression of interferons by
the infected cells.

monocytes , macrophages fibroblasts
also synthesize interferons .

6
Viruses initiate infection by binding to
specific host - cell membrane molecules .

e.g.
1. influenza virus bind to cell membrane
glycoproteins .
2. rhinoviruses bind to intercellular
adhesion molecules (ICAMs).

7
Mechanism of action

Interferons bind to receptors that activate
JAK-STAT pathways.
These induce several genes .
One gene activate a ribonuclease that
degrade viral RNA .

8
2. Other genes activate protein kinases
which inhibit proteinsynthesis .

3. binding of INFs to NK-cells induce
lytic activity .
IL-12 produced by macrophages also
enhance NK-cell activity .

9
Antibody- mediated immunity

Anti-viral antibodies
1. prevent spread during acute infection.
2. protect against reinfection .

10
Protective functions of antibodies

1. secretory IgA blocks viral attachment .
2. complement - fixing antibodies may
cause lysis of enveloped viruses
3.IgM antibody agglutinate viral particles .

11
Cell mediated immunity is important for
control clearance of viral infections .

CTL activity arises within 3 - 4 days,
peak by 7-10 days then decline
when the infection is cleared .

12
Viruses can evade host defenses.

1. Hepatitis C virus
overcome anti - viral effect of INFs
blocking the action of protein kinase.
2.Adenoviruses CMV
reduce surface expression of MHC-1.

13
3. Measles ,CMV HIV reduce MHC
-11 levels .

4. A large no. of viruses cause
generalized immunosuppression.
.
e.g. mumps , measles , EBV., CMV.,
HIV.

14
Influenza virus .
15
Antigenic variation of influenzavirus .

In 1918-1919 an influenza pandemic
killed over 20 million people .
The structure of the virus contain
Hemagglutinins (HA ).
Neuraminidase (NA ).

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17
Shifting Nature of Influenza

Antigenic drift small, ceaseless changes in the
genetic structure. New strains continually
replace old strains.
Antigenic shift major change, usually occurs
when species hosting virus trade viral genes.
Novel strain appears without natural immunity in
host population.

18
1. Antigenic drift gradual minor change in HA
NA.

2. Antigenic shift
sudden major change in HA NA .
( new subtype emerge )

19
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20
1918 Hemagglutinin Causes Severe Lung Damage.
M88/Hsp
M88
Kobasa et al. Nature 2004431703
21
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22

Immunity to bacterial infections.

If the inoculum (dose ) is small and the
virulence of the bacteria is low .
Tissue phagocytes may eliminate
the bacteria .

24
The humoral response (antibody) is the
main protective response against
extracellular bacteria .

Antibodies act in several ways
1. neutralize toxins .
2.activate complement .
- generates anaphylatoxins.
-release chemotactic agents
.

25
Protective functions of antibodies.
26
Intracellular bacteria

Initially activate NK cells which
provide early defense .
Final control is by
cell - mediated immunity .
( this involve activated macrophages )

27
Cell-mediated immunity involve activated
macrophages.
28
Bacteria can by-pass host defense

4 steps in bacterial infections
1. attachment .(adherence).
2. proliferation .
3. invasion of host tissues .
4. toxin - induced damage.

29
Adherence
30
Penetration into the Host Cell
Salmonella entering epithelial cells via invasins
Figure 15.2
31
Secretory IgA block attachment , but some
bacteria secrete proteases that break IgA .

Opsonization phagocytosis prevent
proliferation , but some bacterial
surface structures inhibit phagocytosis,
( polyssacharide capsule ,Strp.pneum.)

32
Strep.pneumonae. Inhibit phagocytosis.
33
3. Some bacteria resist complement lysis .

4. Mycobacteria survive intracellularly by
resisting oxidative attack ,some prevent
lysosomal fusion .

34
Complications of immune responses .

In some cases disease is not caused by
the bacteria but rather by the immune
response.

35
Endotoxins of gram ve bacteriaactivate
macrophages which releasehigh levels of
IL-1, TNF - alpha, these may cause
Septic shock .

In staphylococcal food poisoning ,
enterotoxins act as superantigens
and cause direct massive T-cell
activation . This may cause
Toxic shock syndrome .

36
Endotoxin
Contrast the nature and effects of exotoxins and
endotoxins.
Figure 15.4b
37
Exotoxins
Figure 15.4a
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39
3.Complications of streptococcus pyogenes
throat infections

1. Rheumatic fever antibodies formed against
antigen in the strep. cell wall cross react with
the sacrolemma of
Human heart .Granuloma form in the heart
(Aschoffs
nodules).
2. Rheumatic heart disease repeated attacks
by strep. with different M types can
result in damage to the heart valves.( certain
children have a genetic predisposition
to this immune-mediated disease ). ( high
A.S.O. titer ).

3. Acute glomerulonephritis
antibodies to strep . components combine to
form
immune- complexes which then deposit in the
kidney
glomeruli .

41
4. In chronic intracellular infections e.g.
T.B. excessive CMI responses lead to
granuloma formation .
42
Granuloma formation ( T.B. )
43
The balance between TH1 TH2 is
important in immunity. It determine
the clinical presentation of the
disease .
44
5. Immunological response in leprosy

The response decide the type of disease
1.In tuberculoid leprosy the patient mount an
effective
cell-mediated response.Macrophages destroy the
bacilli
and contain the infection .
2. In lepromatous leprosy the patient is unable
to produce
a cell-mediated response and organisms
multiply and
spread in the tissues gt

Immunity to parasitic infections

A. Protozoal diseases .
These are unicellular organisms .
e.g. malaria , trypansomiasis , toxoplasma,
They have complex life - cycles.
some stages are free in the blood ,
other stages are intracellular.

47
The type of the immune response depend
on the location of the
parasite in the host .

In the blood antibodies may be effective
In the intracellular stage CMI may be
effective.

48
Immunity to Malaria

Caused by genus Plasmodium.
P.falciparum is the most virulent
prevalent.
Infect 10 of the population.
Causes 1 2 million deaths every year.
Have a complex life cycle .

49
Life cycle of malaria
3-stages.
50
During the life- cycle, many antigensappear

Infection begin with mosquito bite.
Sporozoites enter the blood disappear
within 30 min.
Migrate to the liver after 1
week
release merozoites which infect RBCs.

51
Sporozoites stay for only 30 min. in the
blood, therefore induce a poor immune
response.

The intracellular stage in the liver cells
and RBC ,reduce the degree of immune
activation generated by the pathogen.

52
In endemic areas

Only 22 of the children have detectable
antibodies to sporozoites.
In adults 84 have such antibodies.
In general, the degree of immunity to
Malaria is not complete .

53
Trypansomiasis ( sleeping sickness).

As the parasite multiply , an
effective
antibody response develop to
the
glycoprotein coat called variant
surface
glycoprotein (VSG).
These antibodies eliminate most of
the
Parasite from the blood
by
1. complement lysis.
2. opsonization
phagocytosis .

54
Trypansomes, (T. cruz,)
55
However , 1 of the parasite with
differentantigen (VSG ) escape the
antibody response. These
proliferate and a new wave of
parasites invade the blood .

This is called antigenic shifts.
(a characteristic feature of
Trypansomes ).

56
Immunity to parasitic worms (helminths)

Helminths are large multicellular
organisms e.g. Schistosoma (Bilharzia ).
Have complex life- cycle .
Cercaria enter the blood stream and
become schistosomules which enter
capilleries.then pass to the lungs
liver.
then become adult worms.

57
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58
Immune responses are not sufficient
to eliminate the adult worms .

Adult worms evade immune responses
by coating themselves by host
glycoproteins .

59
Humoral immune responses to parasitesare
characterized by

1. elevated IgE.
2. blood eosinophilia .
Eosinophils mediate ADCC to
damage the parasite.

60
A chronic state develop in which
adultworms persist and induce
cell-mediated delayed hypersensitivity
reactions

This eventually result in the formation of
large granulomas .

Immunity to fungi .

Fungal infections of man fall into 4 types
1.superficial mycoses .
2.subcutaneous mycoses.
3.respiratory mycoses.
4.candida albicans .
Recovery is based on cell-mediated immunity.
There is also evidence for neutrophil involvement
In immunity to some respiratory mycoses.

63
Immunology quiz no 4.
64
A.

A12-year old girl has been receiving cytotoxic
drugs for
Acute leukemia. Although there is evidence
that the leukemia is responding, she has become
neutropenic
( neutrophils were less than 0.5 x10 ml )
.Early in the evening she was found to have
fever, within half an hour
she collapsed and was found to have features
of sock
(tachycardia and hypotention ).
Blood was taken for culture which later grew
E. coli. She
was started on antibiotics and fluid
replacement .She
gradually improved during the next 12 hours .